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Genome-Wide Approaches to Dissect the Roles of RNA Binding Proteins in Translational Control: Implications for Neurological Diseases

机译:全基因组方法来分析RNA结合蛋白在翻译控制中的作用:对神经系统疾病的影响。

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Translational control of messenger RNAs (mRNAs) is a key aspect of neurobiology, defects of which can lead to neurological diseases. In response to stimuli, local translation of mRNAs is activated at synapses to facilitate long-lasting forms of synaptic plasticity, the cellular basis for learning and memory formation. Translation, as well as all other aspects of RNA metabolism, is controlled in part by RNA binding proteins (RBPs) that directly interact with mRNAs to form mRNA-protein complexes. Disruption of RBP function is becoming widely recognized as a major cause of neurological diseases. Thus understanding the mechanisms that govern the interplay between translation control and RBP regulation in both normal and diseased neurons will provide new opportunities for novel diagnostics and therapeutic intervention. As a means of studying translational control, genome-wide methods are emerging as powerful tools that have already begun to unveil mechanisms that are missed by single-gene studies. Here, we describe the roles of RBPs in translational control, review genome-wide approaches to examine translational control, and discuss how the application of these approaches may provide mechanistic insight into the pathogenic underpinnings of RBPs in neurological diseases.
机译:信使RNA(mRNA)的翻译控制是神经生物学的一个关键方面,其缺陷可能导致神经系统疾病。响应刺激,在突触处激活mRNA的局部翻译,以促进持久形式的突触可塑性,这是学习和记忆形成的细胞基础。翻译以及RNA代谢的所有其他方面部分受RNA结合蛋白(RBP)的控制,该蛋白直接与mRNA相互作用形成mRNA-蛋白复合物。 RBP功能的破坏已被广泛认为是神经系统疾病的主要原因。因此,了解控制正常和患病神经元中翻译控制和RBP调节之间相互作用的机制将为新颖的诊断和治疗干预提供新的机会。作为研究翻译控制的一种手段,全基因组方法正在成为一种强大的工具,已经开始揭示单基因研究所忽略的机制。在这里,我们描述了RBP在翻译控制中的作用,回顾了全基因组方法来检查翻译控制,并讨论了这些方法的应用如何为神经性疾病中RBP的致病基础提供机理上的见解。

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